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发达国家和发展中国家采用庆大霉素延长给药间隔治疗新生儿败血症

Extended-interval dosing of gentamicin for treatment of neonatal sepsis in developed and developing countries.

作者信息

Darmstadt Gary L, Miller-Bell Mary, Batra Maneesh, Law Paul, Law Kiely

机构信息

Department of International Health, Bloomberg School of Public Health, Johns Hopkins University, Baltimore, MD 21205, USA.

出版信息

J Health Popul Nutr. 2008 Jun;26(2):163-82.

Abstract

Serious bacterial infections are the single most important cause of neonatal mortality in developing countries. Case-fatality rates for neonatal sepsis in developing countries are high, partly because of inadequate administration of necessary antibiotics. For the treatment of neonatal sepsis in resource-poor, high-mortality settings in developing countries where most neonatal deaths occur, simplified treatment regimens are needed. Recommended therapy for neonatal sepsis includes gentamicin, a parenteral aminoglycoside antibiotic, which has excellent activity against gram-negative bacteria, in combination with an antimicrobial with potent gram-positive activity. Traditionally, gentamicin has been administered 2-3 times daily. However, recent evidence suggests that extended-interval (i.e. >24 hours) dosing may be applicable to neonates. This review examines the available data from randomized and non-randomized studies of extended-interval dosing of gentamicin in neonates from both developed and developing countries. Available data on the use of gentamicin among neonates suggest that extended dosing intervals and higher doses (>4 mg/kg) confer a favourable pharmacokinetic profile, the potential for enhanced clinical efficacy and decreased toxicity at reduced cost. In conclusion, the following simplified weight-based dosing regimen for the treatment of serious neonatal infections in developing countries is recommended: 13.5 mg (absolute dose) every 24 hours for neonates of >2,500 g, 10 mg every 24 hours for neonates of 2,000-2,499 g, and 10 mg every 48 hours for neonates of <2,000 g.

摘要

在发展中国家,严重细菌感染是新生儿死亡的最重要单一原因。发展中国家新生儿败血症的病死率很高,部分原因是必要抗生素的使用不足。在大多数新生儿死亡发生的发展中国家资源匮乏、高死亡率环境中,治疗新生儿败血症需要简化的治疗方案。新生儿败血症的推荐治疗方法包括庆大霉素,一种胃肠外氨基糖苷类抗生素,它对革兰氏阴性菌有出色的活性,与一种具有强大革兰氏阳性活性的抗菌药物联合使用。传统上,庆大霉素每日给药2 - 3次。然而,最近的证据表明延长给药间隔(即>24小时)给药可能适用于新生儿。本综述研究了来自发达国家和发展中国家关于新生儿庆大霉素延长给药间隔的随机和非随机研究的现有数据。新生儿使用庆大霉素的现有数据表明,延长给药间隔和更高剂量(>4mg/kg)具有良好的药代动力学特征,有可能提高临床疗效并降低毒性,同时降低成本。总之,建议采用以下基于体重的简化给药方案来治疗发展中国家严重的新生儿感染:体重>2500g的新生儿每24小时13.5mg(绝对剂量),2000 - 2499g的新生儿每24小时10mg,体重<2000g的新生儿每48小时10mg。

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